CD63+ Cancer-Associated Fibroblasts Confer Tamoxifen Resistance to Breast Cancer Cells through Exosomal miR-22
- Adv Sci (Weinh). 2020 Sep 24;7(21):2002518. doi: 10.1002/advs.202002518.
- 1. The State Key Laboratory of Cancer Biology Biotechnology Center School of Pharmacy The Fourth Military Medical University Xi'an 710032 P. R. China.
- 2. Institute of Material Medical School of Pharmacy The Fourth Military Medical University Xi'an 710032 P. R. China.
- 3. Department of General Surgery Tangdu Hospital The Fourth Military Medical University Xi'an 710038 P. R. China.
Tamoxifen remains the most effective treatment for Estrogen receptor α (ERα)-positive breast Cancer. However, many patients still develop resistance to tamoxifen in association with metastatic recurrence, which presents a tremendous clinical challenge. To better understand tamoxifen resistance from the perspective of the tumor microenvironment, the whole microenvironment landscape is charted by single-cell RNA Sequencing and a new cancer-associated fibroblast (CAF) subset, CD63+ CAFs, is identified that promotes tamoxifen resistance in breast Cancer. Furthermore, it is discovered that CD63+ CAFs secrete exosomes rich in miR-22, which can bind its targets, ERα and PTEN, to confer tamoxifen resistance on breast Cancer cells. Additionally, it is found that the packaging of miR-22 into CD63+ CAF-derived exosomes is mediated by SFRS1. Furthermore, CD63 induces STAT3 activation to maintain the phenotype and function of CD63+ CAFs. Most importantly, the pharmacological blockade of CD63+ CAFs with a CD63-neutralizing antibody or cRGD-miR-22-sponge nanoparticles enhances the therapeutic effect of tamoxifen in breast Cancer. In summary, the study reveals a novel subset of CD63+ CAFs that induces tamoxifen resistance in breast Cancer via exosomal miR-22, suggesting that CD63+ CAFs may be a novel therapeutic target to enhance tamoxifen sensitivity.
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Cat. No.Product NameDescriptionTargetResearch Area
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target: JAKResearch Areas: Inflammation/Immunology